Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2

Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2

Channelrhodopsins (ChRs) belong to the unique class of light-gated ion channels. The structure of channelrhodopsin-2 from <i>Chlamydomonas reinhardtii</i> (<i>Cr</i>ChR2) has been resolved, but the mechanistic link between light-induced isomerization of the chromophore retina...

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Main Authors: David Ehrenberg, Nils Krause, Mattia Saita, Christian Bamann, Rajiv K. Kar, Kirsten Hoffmann, Dorothea Heinrich, Igor Schapiro, Joachim Heberle, Ramona Schlesinger
Format: Article
Language:English
Published: MDPI AG 2019-11-01
Series:Applied Sciences
Subjects:
channelrhodopsin
resonance raman
flash photolysis
hybrid qm/mm simulation
electrophysiology
Online Access:https://www.mdpi.com/2076-3417/9/22/4905
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spelling doaj-1318978a34534da58aa4e1817b28c91b2020-11-25T01:33:24ZengMDPI AGApplied Sciences2076-34172019-11-01922490510.3390/app9224905app9224905Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2David Ehrenberg0Nils Krause1Mattia Saita2Christian Bamann3Rajiv K. Kar4Kirsten Hoffmann5Dorothea Heinrich6Igor Schapiro7Joachim Heberle8Ramona Schlesinger9Experimental Molecular Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyGenetic Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyExperimental Molecular Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyMax-Planck-Institute of Biophysics, Max-von-Laue-Straße 3, 60438 Frankfurt am Main, GermanyFritz Haber Center for Molecular Dynamics Research, Institute of Chemistry, Hebrew University of Jerusalem, Jerusalem 9190401, IsraelGenetic Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyGenetic Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyFritz Haber Center for Molecular Dynamics Research, Institute of Chemistry, Hebrew University of Jerusalem, Jerusalem 9190401, IsraelExperimental Molecular Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyGenetic Biophysics, Department of Physics, Freie Universität Berlin, Arnimallee 14, 14195 Berlin, GermanyChannelrhodopsins (ChRs) belong to the unique class of light-gated ion channels. The structure of channelrhodopsin-2 from <i>Chlamydomonas reinhardtii</i> (<i>Cr</i>ChR2) has been resolved, but the mechanistic link between light-induced isomerization of the chromophore retinal and channel gating remains elusive. Replacements of residues C128 and D156 (DC gate) resulted in drastic effects in channel closure. T127 is localized close to the retinal Schiff base and links the DC gate to the Schiff base. The homologous residue in bacteriorhodopsin (T89) has been shown to be crucial for the visible absorption maximum and dark&#8722;light adaptation, suggesting an interaction with the retinylidene chromophore, but the replacement had little effect on photocycle kinetics and proton pumping activity. Here, we show that the T127A and T127S variants of <i>Cr</i>ChR2 leave the visible absorption maximum unaffected. We inferred from hybrid quantum mechanics/molecular mechanics (QM/MM) calculations and resonance Raman spectroscopy that the hydroxylic side chain of T127 is hydrogen-bonded to E123 and the latter is hydrogen-bonded to the retinal Schiff base. The C=N&#8722;H vibration of the Schiff base in the T127A variant was 1674 cm<sup>&#8722;1</sup>, the highest among all rhodopsins reported to date. We also found heterogeneity in the Schiff base ground state vibrational properties due to different rotamer conformations of E123. The photoreaction of T127A is characterized by a long-lived P<sub>2</sub><sup>380</sup> state during which the Schiff base is deprotonated. The conservative replacement of T127S hardly affected the photocycle kinetics. Thus, we inferred that the hydroxyl group at position 127 is part of the proton transfer pathway from D156 to the Schiff base during rise of the P<sub>3</sub><sup>530</sup> intermediate. This finding provides molecular reasons for the evolutionary conservation of the chemically homologous residues threonine, serine, and cysteine at this position in all channelrhodopsins known so far.https://www.mdpi.com/2076-3417/9/22/4905channelrhodopsinresonance ramanflash photolysishybrid qm/mm simulationelectrophysiology
collection DOAJ
language English
format Article
sources DOAJ
author David Ehrenberg
Nils Krause
Mattia Saita
Christian Bamann
Rajiv K. Kar
Kirsten Hoffmann
Dorothea Heinrich
Igor Schapiro
Joachim Heberle
Ramona Schlesinger
spellingShingle David Ehrenberg
Nils Krause
Mattia Saita
Christian Bamann
Rajiv K. Kar
Kirsten Hoffmann
Dorothea Heinrich
Igor Schapiro
Joachim Heberle
Ramona Schlesinger
Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2
Applied Sciences
channelrhodopsin
resonance raman
flash photolysis
hybrid qm/mm simulation
electrophysiology
author_facet David Ehrenberg
Nils Krause
Mattia Saita
Christian Bamann
Rajiv K. Kar
Kirsten Hoffmann
Dorothea Heinrich
Igor Schapiro
Joachim Heberle
Ramona Schlesinger
author_sort David Ehrenberg
title Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2
title_short Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2
title_full Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2
title_fullStr Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2
title_full_unstemmed Atomistic Insight into the Role of Threonine 127 in the Functional Mechanism of Channelrhodopsin-2
title_sort atomistic insight into the role of threonine 127 in the functional mechanism of channelrhodopsin-2
publisher MDPI AG
series Applied Sciences
issn 2076-3417
publishDate 2019-11-01
description Channelrhodopsins (ChRs) belong to the unique class of light-gated ion channels. The structure of channelrhodopsin-2 from <i>Chlamydomonas reinhardtii</i> (<i>Cr</i>ChR2) has been resolved, but the mechanistic link between light-induced isomerization of the chromophore retinal and channel gating remains elusive. Replacements of residues C128 and D156 (DC gate) resulted in drastic effects in channel closure. T127 is localized close to the retinal Schiff base and links the DC gate to the Schiff base. The homologous residue in bacteriorhodopsin (T89) has been shown to be crucial for the visible absorption maximum and dark&#8722;light adaptation, suggesting an interaction with the retinylidene chromophore, but the replacement had little effect on photocycle kinetics and proton pumping activity. Here, we show that the T127A and T127S variants of <i>Cr</i>ChR2 leave the visible absorption maximum unaffected. We inferred from hybrid quantum mechanics/molecular mechanics (QM/MM) calculations and resonance Raman spectroscopy that the hydroxylic side chain of T127 is hydrogen-bonded to E123 and the latter is hydrogen-bonded to the retinal Schiff base. The C=N&#8722;H vibration of the Schiff base in the T127A variant was 1674 cm<sup>&#8722;1</sup>, the highest among all rhodopsins reported to date. We also found heterogeneity in the Schiff base ground state vibrational properties due to different rotamer conformations of E123. The photoreaction of T127A is characterized by a long-lived P<sub>2</sub><sup>380</sup> state during which the Schiff base is deprotonated. The conservative replacement of T127S hardly affected the photocycle kinetics. Thus, we inferred that the hydroxyl group at position 127 is part of the proton transfer pathway from D156 to the Schiff base during rise of the P<sub>3</sub><sup>530</sup> intermediate. This finding provides molecular reasons for the evolutionary conservation of the chemically homologous residues threonine, serine, and cysteine at this position in all channelrhodopsins known so far.
topic channelrhodopsin
resonance raman
flash photolysis
hybrid qm/mm simulation
electrophysiology
url https://www.mdpi.com/2076-3417/9/22/4905
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